The synthesis of C11N5 marine sponge alkaloids (±)-hymenin (1), stevensine (2), hymenialdisine (3), and debromohymenialdisine (4) is described. These natural products are the primary family members of the sponge metabolites that contain a fused pyrrolo[2,3-c]lazepin-8-one ring system with either a 2-aminoimidazole (AI) or glycocyamidine appendage. The key steps in the synthesis centered around the generation of novel azafulvenium ions and their regioselective heterodimerization with AI in order to create the tricyclic core. A rarely used protodebromination/oxidation strategy was employed to selectively generate the desired a-bromo substitution pattern seen in hymenialdisine (3). In addition, the AI moiety was shown to be a useful precursor to the glycocyamidine unit found in 3 and 4, which suggests that AI derived natural products may be the biogenic forerunners to glycocyamidine metabolites.
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机译:C 11 N 5 海洋海绵生物碱(±)-处女膜素(1),stevensine(2),hymenialdisine(3)和debromohymenialdisine(4)的合成为描述。这些天然产物是海绵代谢物的主要家族成员,其中包含稠合的吡咯并2,3-c-lazepin-8-环系统,带有2-氨基咪唑(AI)或糖嘧啶附属物。合成过程中的关键步骤集中在新型氮杂富烯鎓离子的产生及其与AI的区域选择性异二聚化反应上,以创造三环核。采用了很少使用的原去溴化/氧化策略来选择性地产生在膜虫碱中看到的所需的α-溴取代模式(3)。另外,显示出AI部分是在3和4中发现的糖嘧啶单元的有用前体,这表明AI衍生的天然产物可能是糖嘧啶代谢物的生物先驱。
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